JP5758904B2 - Nitrite pharmaceutical formulations and their use - Google Patents

Description

  The present invention relates to nitrite pharmaceutical compositions and medical uses of these compositions.

  Chronic tissue ischemia (i.e., continually restricting blood supply to a particular tissue) can impair tissue function and damage tissue and organs. Chronic tissue ischemia thus significantly contributes to human morbidity and mortality. Chronic tissue ischemia is a wide range of medical conditions that result in persistent or recurrent limitations of blood supply to the tissue [eg, peripheral arterial disease, type 1 diabetes, type 2 diabetes, atherosclerotic cardiovascular disease , Intermittent claudication, critical limb ischemic disease, stroke, myocardial infarction, inflammatory bowel disease and peripheral neuropathy; wounds, burns, lacerations, bruises, fractures, infections or surgical procedures Trauma such as hernia, congenital malformations such as cardiac defect and gastrointestinal defect]. Thus, chronic tissue ischemia can occur in various types of tissues including, for example, skeletal muscle, smooth muscle, myocardium, nerve tissue, skin, mesenchymal tissue, connective tissue, gastrointestinal tissue and bone.

  Accordingly, there is a continuing need for treatment methods that restore the blood supply to the lesion site.

  In general, in a first aspect, the present invention is directed to a pharmaceutical composition comprising an effective amount of inorganic nitrite or a pharmaceutically acceptable salt, solvate or prodrug thereof and a pharmaceutically acceptable excipient. . Preferably, by administering the pharmaceutical composition to a human, the plasma concentration of nitrite ion is 0.05 μM to 10 μM (e.g., 0.1 μM to 10 μM, 0.5 μM to 5 μM, 0.1 μM to 3 μM, over a maximum of 14 hours). Or 0.1 μM to 1 μM).

  In another embodiment, the inorganic nitrite is 0.1 μg to 10 mg / kg human body weight (e.g., 1 μg to 5 mg / kg, 0.05 to 10 mg / kg, 0.1 to 5 mg / kg, 0.5 to 5 mg / kg, 0.5 to 3 mg). / kg, 0.1-1.5 mg / kg, 0.1-0.35 mg / kg, 0.35-0.75 mg / kg, or 0.75-1 mg / kg). In yet another embodiment, the dose is 0.25 mg / kg, 0.5 mg / kg or 1 mg / kg.

In certain embodiments, the pharmaceutical composition comprises 0.5-5.0 mmol (eg, 1.0-4.0 mmol) nitrite ions (NO ₂ ⁻ ).

In another embodiment, nitrous nitrate ions are provided as NaNO _2, KNO ₂ or nitrous acid arginine. In certain embodiments, nitrous nitrate ions are provided as NaNO _2.

  In yet another embodiment, the pharmaceutical composition is formulated for oral administration. In a further embodiment, the pharmaceutical composition is a tablet or capsule.

  In another embodiment, the pharmaceutical composition is an application that is an alkalinizing agent, glidant, lubricant, bulking agent, cellulose-containing polymer or polyethylene glycol or any combination thereof. Contains form. In yet another embodiment, the pharmaceutical composition comprises a pharmaceutically acceptable excipient (e.g., a pH sensitive polymer or a biodegradable polymer) for delayed release of the inorganic nitrite, Thus, when administered orally to a human subject, the inorganic nitrite is not substantially released in the stomach of the human subject. In a further embodiment, the enteric coating comprises a pharmaceutically acceptable excipient for delayed release of the inorganic nitrite. In certain embodiments, the pharmaceutically acceptable excipient is ethyl cellulose, cellulose acetate, cellulose acetate butyrate, cellulose triacetate, cellulose acetate phthalate (CAP), cellulose trimellitate, hydroxypropylmethylcellulose succinate or “ Eudragit (registered trademark) L "or" Eudragit (registered trademark) S ". In a further embodiment, the pharmaceutical composition further comprises polyethylene glycol and / or a plasticizer.

  In some embodiments, the pharmaceutical composition is a multiparticulate dosage form. In certain embodiments, the multiparticulate dosage form includes pellets or granules. In a further embodiment, the pellet or granule is a biodegradable polymer (e.g., a polysaccharide such as alginate, pectin, carrageenan, chitosan, dextran, shellac, or xanthan gum, or any mixture thereof). Coated with a coating layer containing.

  In a second aspect, the present invention comprises an effective amount of an inorganic nitrite or a pharmaceutically acceptable salt, solvate or prodrug thereof and a pharmaceutically acceptable excipient for delayed release of the inorganic nitrite ( Thereby, when administered orally to a human subject, the inorganic nitrite is not substantially released in the stomach of the human subject) and relates to a pharmaceutical composition formulated for oral administration. In certain embodiments, the pharmaceutical composition is a tablet or capsule.

  In a third aspect, the invention is suitable for oral administration comprising (a) an effective amount of inorganic nitrite or a pharmaceutically acceptable salt, solvate or prodrug thereof; and (b) an enteric coating layer. The target pharmaceutical composition is intended. Preferably, the pharmaceutical composition is formulated such that when administered to a human subject, the inorganic nitrite is not substantially released in the stomach of the human subject.

  In certain embodiments, administration of the pharmaceutical composition to a human results in a plasma concentration of 0.05 μM to 10 μM (e.g., 0.1 μM to 10 μM, 0.5 μM to 5 μM, 0.1 μM to 3 μM, or 0.1 μM to 1 μM). Maintained.

  In another embodiment, the inorganic nitrite is 0.1 μg to 10 mg / kg human body weight (e.g., 1 μg to 5 mg / kg, 0.05 to 10 mg / kg, 0.1 to 5 mg / kg, 0.5 to 5 mg / kg, 0.5 to 3 mg). / kg, 0.1-1.5 mg / kg, 0.1-0.35 mg / kg, 0.35-0.75 mg / kg, or 0.75-1 mg / kg). In yet another embodiment, the dose is 0.25 mg / kg, 0.5 mg / kg or 1 mg / kg.

In yet another embodiment, the pharmaceutical composition comprises 0.5-5.0 mmol (eg, 1.0-4.0 mmol) nitrite ions (NO ₂ ⁻ ).

In certain embodiments, nitrous nitrate ions are provided as NaNO _2, KNO ₂ or nitrous acid arginine. In a further embodiment, nitrous nitrate ions are provided as NaNO _2.

  In another embodiment, the enteric coating layer comprises a pharmaceutically acceptable excipient, where the excipient is a pH sensitive polymer or a biodegradable polymer.

  In yet another embodiment, the pharmaceutical composition is a tablet or capsule.

  In any of the above embodiments, the plasma concentration of nitrite ions is maintained for up to 14 hours (eg, 4-14 hours, 6-12 hours, or 6-10 hours). The period during which the plasma concentration is maintained can be, for example, during and / or after the time when the plasma concentration is at its peak. In some embodiments, 30-50% of the nitrite ions are released in the first hour and the remainder of the nitrate ions are released in the next 2-14 hours.

  In another aspect, the present invention is directed to a method of treating or preventing chronic tissue ischemia in a human. Preferably, the method comprises administering to the human any of the pharmaceutical compositions described herein. In certain embodiments, the administration is oral.

  In yet another aspect, the present invention is directed to a method of compensating for the lack of circulating nitrite found in a patient's body, wherein the method comprises any of the pharmaceutical compositions described herein in humans. Administration.

  The present invention relates to pharmaceutical compositions of nitrites (e.g., inorganic nitrites) and the like for treating chronic tissue ischemia, including chronic tissue ischemia associated with disease, trauma or birth defects. It relates to the use of the composition.

  As used herein, the term `` delayed release '' is a pharmaceutical preparation that passes through the stomach substantially intact and dissolves in the small and / or large intestine (e.g., the colon) ( For example, oral administration preparation). In some embodiments, delayed release of the active agent (eg, nitrite described herein) is by using an enteric coating of an oral drug (eg, an oral dosage form).

  The term “effective amount” of an agent, as used herein, is an amount sufficient to produce a beneficial or desirable result, such as a clinical result, and as such, “ An “effective amount” depends on the context in which the term is used.

  The terms `` extended release '' or `` sustained release '' are synonymous and mean that a drug is prolonged (e.g. 6-12 hours or longer) compared to an immediate release formulation of the same drug Means a drug formulation that gradually releases over time. Preferably, although not required, a substantially constant blood concentration of the drug over an extended period of time (this is within the therapeutic level and peak plasma concentration ranges such as 0.05-10 μM, 0.1-10 μM, In the range of 0.1-5.0 μM or 0.1-1 μM).

  As used herein, the terms “formulated for enteric release” and “enteric formulation” are used in the strongly acidic (low pH) environment of the stomach. Means a pharmaceutical composition for oral administration (eg, an oral dosage form) that can provide protection from dissolution in Enteric preparations can be obtained, for example, by incorporating into the pharmaceutical composition a polymer that is resistant to dissolution in gastric juice. In some embodiments, the optimum pH for dissolution of the polymer is in the range of about 5.0 to 7.0 (“pH sensitive polymer”). Representative polymers include `` Eudragit (registered trademark) '' (e.g., `` Eudragit (registered trademark) L100 '', `` Eudragit (registered trademark) S100 '', `` Eudragit (registered trademark) L-30D '', `` Eudragit (registered trademark) (Trademark) FS 30D '' and `` Eudragit® L100-55 ''), known as trade names of methacrylic acid copolymer, cellulose acetate phthalate, cellulose acetate trimellitic acid, polyvinyl acetate phthalate (e.g., `` Coateric® ) "), Hydroxyethylcellulose phthalate, hydroxypropylmethylcellulose phthalate, shellac, or an aqueous dispersion thereof. Examples of the aqueous dispersion of the polymer include a dispersion of cellulose acetate phthalate (“Aquateric®”) and a dispersion of shellac (for example, “MarCoat 125” and “MarCoat 125N”). The enteric formulation is at least 50%, at least 60%, at least 70%, at least 80%, at least 90%, at least 95% released into the stomach at the administered dose compared to the immediate release formulation. %, Or even at least 98%. When a tablet or capsule is coated with such a polymer, the coating is also referred to as an “enteric coating”.

  The term “pharmaceutical composition” as used herein refers to a compound described herein (eg, inorganic nitrite or any pharmaceutically acceptable salt, solvate or prodrug thereof. ) And is formulated with pharmaceutically acceptable excipients and is typically approved by government supervisors as part of a therapeutic regimen for treating mammalian diseases. It means a composition that is obtained, manufactured and sold. The pharmaceutical composition can be formulated, for example, for oral administration in unit dosage form (eg, tablet, capsule, caplet, gelcap or syrup); for topical administration ( Can be formulated (eg, as a cream, gel, lotion, or ointment); includes a granular embolus in a solvent system suitable for intravenous administration (eg, suitable for intravenous use) Not as a sterile solution); or it can be formulated into any other dosage form described herein.

  “Pharmaceutically acceptable excipient” as used herein is described herein, which has the property of being non-toxic and non-inflammatory in the body of a patient. Means any component other than the compound (eg, a vehicle capable of suspending or dissolving the active compound). Excipients can include, for example: anti-adhesives, antioxidants, binders, coatings, compression aids, disintegrants, dyes (colorants), emollients Agents, emulsifiers, extenders (diluents), film formers or film coating agents, flavors, fragrances, glidants (flow enhancers), lubricants Preservatives, printing inks, adsorbents, suspending or dispersing agents, sweeteners, or waters of hydration. Exemplary excipients include, but are not limited to, butylated hydroxytoluene (BHT), calcium carbonate, calcium phosphate (dibasic), calcium stearate, croscarmellose, Cross-linked polyvinyl pyrrolidone, citric acid, crospovidone, cysteine, ethyl cellulose, gelatin, hydroxypropyl cellulose, hydroxypropyl methylcellulose, lactose, magnesium stearate, maltitol, maltose, mannitol, methionine, methylcellulose, methylparaben, microcrystalline cellulose, polyethylene glycol , Polyvinylpyrrolidone, povidone, alpha starch, propylparaben, retinyl palmitate, shellac, silicon dioxide, sodium carboxymethyl Cellulose, sodium citrate, sodium starch glycolate, sorbitol, starch (corn), stearic acid, stearic acid, sucrose, talc, titanium dioxide, vitamin A, vitamin E, vitamin C, and xylitol.

  The term “pharmaceutically acceptable prodrug” as used herein does not have undue toxicity, irritation, allergic response, etc., corresponds to a reasonable benefit / risk ratio, and Prodrugs of the compounds of the present invention suitable for use in contact with human and animal tissues within the scope of sound medical judgment, effective for their intended use, and possible In the case, it means the zwitterionic form of the compound of the invention.

  The term “pharmaceutically acceptable salt” as used herein is sound, without excessive toxicity, irritation, allergic response, etc., and corresponding to a reasonable benefit / risk ratio. Means a salt that is suitable for use in contact with human and animal tissues within the scope of such medical judgment. Pharmaceutically acceptable salts are well known in the art. For example, pharmaceutically acceptable salts are described in `` Berge et al., J. Pharmaceutical Sciences 66: 1-19, 1977 '' and `` Pharmaceutical Salts: Properties, Selection, and Use, (Eds. PH Stahl and CG Wermuth), Wiley-VCH, 2008 ". The salts can be prepared in situ during the final isolation and purification of the compounds of the invention, or independently the base group can be attached to a suitable organic acid or inorganic It can be prepared by reacting with an acid. Representative acid addition salts include acetate, adipate, alginate, ascorbate, aspartate, benzenesulfonate, benzoate, bisulfate, borate, butyrate, camphorate, Camphor sulfonate, citrate, cyclopentanepropionate, digluconate, dodecyl sulfate, ethane sulfonate, fumarate, glucoheptonate, glycerophosphate, hemisulfate, heptonate , Hexanoate, hydrobromide, hydrochloride, hydroiodide, 2-hydroxy-ethanesulfonate, lactobionate, lactate, laurate, lauryl sulfate, malate, maleic acid Salt, malonate, methanesulfonate, 2-naphthalenesulfonate, nicotinate, nitrate, oleate, oxalate, palmitate, pamo Acid, pectate, persulfate, 3-phenylpropionate, phosphate, picrate, pivalate, propionate, stearate, succinate, sulfate, tartrate, thiocyanate Salt, toluenesulfonate, undecanoate, valerate, and the like. Representative alkali metal salts or alkaline earth metal salts include sodium cation, lithium cation, potassium cation, calcium cation, magnesium cation, etc., and non-toxic ammonium cation, quaternary ammonium cation and amine cation (these Includes, but is not limited to, ammonium, tetramethylammonium, tetraethylammonium, methylamine, dimethylamine, trimethylamine, triethylamine, ethylamine, and the like.

  The term “pharmaceutically acceptable solvate” or “solvate” as used herein means a compound of the invention in which a molecule of a suitable solvent is incorporated in its crystal lattice. To do. A suitable solvent is physiologically tolerable at the dosage administered. For example, solvates can be prepared by crystallization, recrystallization, or precipitation from a solution containing an organic solvent, water, or a mixture thereof. Examples of suitable solvents are ethanol, water (e.g. monohydrate, dihydrate and trihydrate), N-methylpyrrolidinone (NMP), dimethyl sulfoxide (DMSO), N, N'-dimethylformamide (DMF), N, N'-dimethylacetamide (DMAC), 1,3-dimethyl-2-imidazolidinone (DMEU), 1,3-dimethyl-3,4,5,6-tetrahydro-2- (1H ) -Pyrimidinone (DMPU), acetonitrile (ACN), propylene glycol, ethyl acetate, benzyl alcohol, 2-pyrrolidone, benzyl benzoate, and the like. When water is the solvent, the solvate is referred to as a “hydrate”.

  The term “prevent”, as used herein, prevents prophylaxis of one or more symptoms or conditions of a disease, disorder or condition described herein (eg, chronic tissue ischemia). Means treatment or treatment. Treatment can be initiated, for example, prior to an event that precedes the onset of the disease, disorder, or condition (“pre-exposure onset prevention”) or after such an event (“post-exposure onset prevention”). Treatment involving administering a compound of the invention or pharmaceutical composition thereof may be acute, short term or long term. The dose administered can vary during the course of prophylactic treatment.

The term “prodrug” as used herein means a compound that is rapidly transformed in vivo to the parent compound represented by the formula above. Prodrugs also include biologically equivalent compounds that form nitrite ions (NO ₂ ⁻ ) or nitrous oxide (NO) in the body when administered to humans. `` T. Higuchi and V. Stella, Pro-drugs as Novel Delivery Systems, Vol. 14 of the ACS Symposium Series '' and `` Edward B. Roche, ed., Bioreversible Carriers in Drug Design, American Pharmaceutical Association and Pergamon Press, 1987 Are fully discussed (each of which is incorporated herein by reference). Preferably, prodrugs of the compounds of the invention are pharmaceutically acceptable, such as those described in EP 1336602A1, which is incorporated herein by reference.

  As used herein, and as well understood in the art, “treatment” is an approach for obtaining beneficial or desirable results, such as clinical results. . Beneficial or desirable results may include, but are not limited to, the following: reduction or improvement of one or more symptoms or conditions; reduction of the degree of a disease, disorder or condition; disease, disorder or condition A stabilized (ie, not exacerbated) state of the disease; prevention of the spread of the disease, disorder or condition; delay or slowing the progression of the disease, disorder or condition; improvement or alleviation of the disease, disorder or condition; And a detectable or undetectable remission (partial or comprehensive). “Treatment” also means prolonging survival as compared to expected survival if not receiving treatment. As used herein, the terms “treating” and “treatment” refer to a disease or condition to which the term applies or one or more symptoms of such a disease or condition. Delay the onset, delay or reverse the progression of the disease or condition to which the term applies or one or more symptoms of such disease or condition, or the disease or condition to which the term applies or such It may also mean reducing one or more symptoms of the disease or condition.

  The term `` unit dosage form '' refers to a physically separated unit suitable for unit administration to a human subject and another mammal, wherein each unit is any suitable type or Means a predetermined amount of active substance calculated to produce the desired therapeutic effect in cooperation with multiple types of pharmaceutical excipients).

  As used herein, the term “plasma concentration” refers to the amount of nitrite ions present in the plasma of a treated subject (eg, using the assay described below). The amount of nitrite ions measured in rabbits, or the amount of nitrite ions in the human body).

  Other features and advantages of the invention will be apparent from the following detailed description, drawings, and claims.

FIG. 1 is a diagram showing the results obtained from a simulation experiment of nitrite plasma concentration derived from the controlled release preparation (1). FIG. 2 is a view showing the results obtained from a simulation experiment of nitrite plasma concentration derived from the controlled release preparation (2). FIG. 3 is a view showing the results obtained from a simulation experiment of nitrite plasma concentration derived from the controlled release preparation (5). FIG. 4 is a diagram showing the results obtained from a simulation experiment of nitrite plasma concentration derived from the controlled release preparation (9). FIG. 5 is a diagram showing the results obtained from a simulation experiment of nitrite plasma concentration derived from the controlled release preparation (9C). FIG. 6 is a diagram showing the results obtained from a simulation experiment of nitrite plasma concentration derived from a controlled release formulation (10C). FIG. 7 is a view showing the results obtained from a simulation experiment of nitrite plasma concentration derived from the controlled release preparation (12). FIG. 8 is a diagram showing the results obtained from a simulation experiment of nitrite plasma concentration derived from the controlled release preparation (12C). FIG. 9 is a view showing the results obtained from a simulation experiment of nitrite plasma concentration derived from the controlled release preparation (13). FIG. 10 shows the results obtained from a simulated nitrite plasma concentration derived from a control immediate release formulation. FIG. 11 shows the total NOx release profile for formulation (100A), formulation (200A) and formulation (300A) in the rabbit body. FIG. 12 shows the release profiles of nitrate, nitrosothiols, nitrosoheme and nitrosamines for formulation (100A), formulation (200A) and formulation (300A) in the rabbit body. FIG. 13 shows the release profile of free nitrite for formulation (100A), formulation (200A) and formulation (300A) in the rabbit body.

  The present invention may administer a physiologically acceptable composition of nitrite (e.g., inorganic nitrite) and a patient diagnosed as suffering from, for example, chronic tissue ischemic disease. Target method.

Nitrite
Inorganic nitrite The pharmaceutically acceptable composition of the present invention comprises an inorganic nitrite [eg, a salt or ester of nitrous acid (HNO ₂ )] or a pharmaceutically acceptable salt thereof. Nitrites may include, but are not limited to: alkali metal (eg, sodium, potassium) salts; alkaline earth metal (eg, calcium, magnesium and barium) salts; and Salts of organic bases (eg amine bases) and inorganic bases. The compounds of the present invention also include all isotopes of atoms occurring in the intermediates or final compounds. Isotopes include those atoms having the same atomic number but different mass numbers. For example, isotopes of hydrogen include tritium and deuterium. The term “compound” as used herein in connection with any inorganic nitrite or a pharmaceutically acceptable salt, solvate or prodrug thereof. All compounds and pharmaceutically acceptable salts thereof are also intended to encompass solvated (eg hydrated) forms. Nitrite is represented by the chemical formula “NO ₂ ⁻ ” and can exist as ions in water. Sodium nitrite is represented by the chemical formula “NaNO ₂ ” and typically dissolves in water to form sodium ions “Na ⁺ ” and nitrite ions “NO ₂ ⁻ ”. It is further understood that the invention encompasses all such solvated forms (eg, hydrates) of nitrite compounds. Exemplary nitrite compounds are described in WO 2008/105730, which is incorporated herein by reference.

In addition to sodium nitrite, typical inorganic nitrite compounds include the following: ammonium nitrite (NH ₄ NO ₂ ), barium nitrite (Ba (NO ₂ ) ₂ ; for example, anhydrous nitrous acid Barium or barium nitrite monohydrate), calcium nitrite (Ca (NO ₂ ) ₂ ; for example, anhydrous calcium nitrite or calcium nitrite monohydrate), cesium nitrite (CsNO ₂ ), cobalt nitrite ( II) (Co (NO ₂ ) ₂ ), potassium cobalt (III) nitrite (CoK ₃ (NO ₂ ) ₆ ; for example, cobalt (III) potassium sesquihydrate), lithium nitrite (LiNO ₂ ; , Anhydrous lithium nitrite or lithium nitrite monohydrate), magnesium nitrite (MgNO ₂ ; eg, magnesium nitrite trihydrate), potassium nitrite (KNO ₂ ), rubidium nitrite (RbNO ₂ ), silver nitrite (I) (AgNO _2), nitrous acid strontium _{(Sr (NO 2) 2)} , and nitrous Zinc _{(Zn (NO 2) 2)} .

The compounds of the present invention can be prepared in a variety of ways known to one skilled in the art of chemical synthesis. Methods for preparing nitrites are well known in the art and a wide range of precursors and nitrites are readily available commercially. Alkali metal and alkaline earth metal nitrites can be synthesized by reacting a mixture of nitric oxide (NO) and nitrogen dioxide (NO ₂ ) with the corresponding metal hydroxide solution, and It can also be synthesized by subjecting the corresponding nitrate to thermal decomposition. Other nitrites can be obtained by reducing the corresponding nitrates.

  The compounds of this invention can be prepared from readily available starting materials using methods and procedures known in the art. Where typical or preferred process conditions (i.e. reaction temperature, reaction time, reactant molar ratio, solvent, pressure, etc.) are given, other process conditions can be used unless otherwise indicated. It will be understood that there is. Optimum reaction conditions may vary with the particular reactants or solvent used, but such conditions can be determined by one skilled in the art by routine optimization procedures.

  Suitable pharmaceutically acceptable salts include, for example, sodium nitrite, potassium nitrite or calcium nitrite. Representative additional salts are described in `` Remington's Pharmaceutical Sciences, 17th ed., Mack Publishing Company, Easton, Pa., 1985, p. 1418 '', `` Berge et al., J. Pharmaceutical Sciences 66: 1-19, 1977 '' and `` Pharmaceutical Salts: Properties, Selection, and Use, (Eds. PH Stahl and CG Wermuth), Wiley-VCH, 2008 '' (each of which is herein incorporated by reference in its entirety. Embedded in).

Pharmaceutical Compositions The pharmaceutically acceptable compositions of the present invention comprise an inorganic nitrite (eg, a salt of nitrous acid (HNO ₂ ), eg, NaNO ₂ ) or a pharmaceutically acceptable salt, solvate or prodrug thereof. Including. When used as a medicament, any of the compounds of the present invention can be administered in the form of a pharmaceutical composition. These compositions can be prepared by methods well known in the pharmaceutical art, and depending on whether local or systemic therapy is desired and on the area to be treated Can be administered by various routes. Administration is local administration, parenteral administration, intravenous administration, intraarterial administration, subcutaneous administration, intramuscular administration, intracranial administration, intraorbital administration, intraocular administration, intraventricular administration, intracapsular administration, intrathecal administration, tank Internal administration, intraperitoneal administration, intranasal administration, aerosol administration, suppository administration or oral administration may be used.

  The present invention further encompasses pharmaceutical compositions that can include one or more pharmaceutically acceptable carriers. In preparing the pharmaceutical compositions of the present invention, the active ingredient is typically mixed with an excipient, diluted with an excipient, or in the form of, for example, a capsule, sachet, paper or another container. Enclose in a carrier. When an excipient is used as a diluent, it can be a solid, semi-solid or liquid material (eg, normal saline) and acts as a vehicle, carrier or vehicle for the active ingredient. Thus, the composition is in the form of tablets, powders, lozenges, sachets, cachets, elixirs, suspensions, emulsions, solutions, syrups, soft gelatin capsules and hard gelatin capsules. be able to. As is known in the art, the type of diluent can vary depending on the intended route of administration. The composition thus obtained can also contain additional agents such as preservatives.

The therapeutic agents of the invention can be administered alone or in admixture in the presence of a pharmaceutically acceptable excipient or carrier. The excipient or carrier is selected based on the method of administration and the route of administration. Suitable pharmaceutical carriers and essential pharmaceutical substances for use in pharmaceutical formulations are described in `` Remington: The Science and Practice of Pharmacy, 21 ^st Ed., Gennaro, Ed., Lippencott Williams & Wilkins (2005) '' (This is a well-known reference text in the field) and “USP / NF (United States Pharmacopeia and the National Formulary)”. In preparing a formulation, the active compound can be milled to a suitable particle size prior to combining with the remaining ingredients. If the active compound is substantially insoluble, it can be ground to a particle size of less than 200 mesh. If the active compound is substantially water soluble, the particle size can be adjusted by milling to provide a substantially homogeneous distribution in the formulation (eg, about 40 mesh).

Examples of suitable excipients are lactose, dextrose, sucrose, sorbitol, mannitol, starches, gum arabic, calcium phosphate, alginates, gum tragacanth, gelatin, calcium silicate, microcrystalline cellulose, polyvinylpyrrolidone, cellulose, water, Syrup and methylcellulose. The formulation may additionally contain: smoothing agents such as talc, magnesium stearate and mineral oil; wetting agents; emulsifiers and suspending agents; preservatives such as methyl hydroxybenzoate. And hydroxypropyl benzoate; sweeteners; and flavoring agents. Another representative of the excipients are described in the ^{"Handbook of Pharmaceutical Excipients, 6 th Edition} , Rowe et al., Eds., Pharmaceutical Press (2009) ".

The pharmaceutical composition may contain nitrate or a prodrug thereof or another therapeutic agent. Representative nitrates are described in WO 2008/105730. Exemplary therapeutic agents that can be included in the compositions described herein include therapeutics (e.g., antithrombotic agents (e.g., dipyridamole, clopidogrel, etc.), antihypertensive agents (e.g. For example, Ca ⁺⁺ channel blockers, AT-2 blockers, ACE inhibitors, etc.), anticholesterol drugs (eg, statins, fibrates, etc.) and thiazolidinedione therapeutic agents.

  The pharmaceutical composition is formulated so as to release the active ingredient immediately or over a long period of time or delayed release using methods known in the art after administration to a patient. Can be

  The composition can be formulated in unit dosage form, each dosage containing for example 0.1-500 mg of active ingredient. For example, the dosage is about 0.1 mg to about 50 mg, about 0.1 mg to about 40 mg, about 0.1 mg to about 20 mg, about 0.1 mg to about 10 mg, about 0.2 mg to about 20 mg, about 0.3 mg to about 15 mg, about 0.4 mg to about 10 mg, about 0.5 mg to about 1 mg, about 0.5 mg to about 100 mg, about 0.5 mg to about 50 mg, about 0.5 mg to about 30 mg, about 0.5 mg to about 20 mg, about 0.5 mg to about 10 mg, about 0.5 mg to about 5 mg, about 1 mg to about 50 mg, about 1 mg to about 30 mg, about 1 mg to about 20 mg, about 1 mg to about 10 mg, about 1 mg to about 5 mg, about 5 mg to about 50 mg, about 5 mg to about 20 mg, about 5 mg to about 5 mg About 10 mg, about 10 mg to about 100 mg, about 20 mg to about 200 mg, about 30 mg to about 150 mg, about 40 mg to about 100 mg, about 50 mg to about 100 mg active ingredient, about 50 mg to about 300 mg, about 50 mg to about 250 mg, about 100 mg To about 300 mg, or about 100 mg to about 250 mg of active ingredient. To prepare a solid composition such as a tablet, the principal active ingredient is mixed with one or more pharmaceutical excipients to form a solid bulk pharmaceutical composition comprising a homogeneous mixture of the compounds of the invention. When these bulk pharmaceutical compositions are referred to as homogeneous, the active ingredient is typically a composition so that the composition can be easily divided into equally effective unit dosage forms such as tablets or capsules. Uniformly distributed throughout. This solid bulk formulation is then divided into unit dosage forms of the type described above containing, for example, 0.1 to about 500 mg of the active ingredient of the present invention.

Compositions for oral administration Pharmaceutical compositions contemplated by the present invention include pharmaceutical compositions formulated for oral administration ("oral dosage forms"). Oral dosage forms are, for example, tablets, capsules, liquid solutions or suspensions containing the active ingredient (s) in admixture with non-toxic pharmaceutically acceptable excipients. Can be in the form of a powder or liquid or solid crystals. These excipients can be, for example, inert diluents or extenders (eg sucrose, sorbitol, sugar, mannitol, microcrystalline cellulose, starches such as potato starch, calcium carbonate , Sodium chloride, lactose, calcium phosphate, calcium sulfate, or sodium phosphate); granulating and disintegrating agents (eg, cellulose derivatives such as microcrystalline cellulose, starches such as potato starch, croscarmellose sodium, Alginate or alginic acid); binder (eg sucrose, glucose, sorbitol, gum arabic, alginic acid, sodium alginate, gelatin, starch, alpha starch, microcrystalline cellulose, magnesium magnesium silicate, carboxyme Sodium cellulose, methylcellulose, hydroxypropylmethylcellulose, ethylcellulose, polyvinylpyrrolidone, or polyethylene glycol); and smoothing agents, glidants and anti-adhesive agents (eg, magnesium stearate, zinc stearate, stearic acid, silica, cured) Vegetable oil or talc). Other pharmaceutically acceptable excipients can be colorants, flavoring agents, plasticizers, humectants, buffering agents, and the like.

  Formulations for oral administration are as chewable tablets or hard gelatin capsules, where the active ingredient is an inert solid diluent (e.g. potato starch, lactose, microcrystalline cellulose, calcium carbonate, calcium phosphate, or Or as a soft gelatin capsule (where the active ingredient is mixed with water or an oily medium (e.g., peanut oil, animal paraffin or olive oil)). Can also be provided. Powders, granules and pellets use the ingredients listed above under tablets and capsules, in a customary manner, for example using a mixer, fluid bed apparatus or spray drying apparatus etc. Can be prepared.

  Controlled release compositions for oral use can be constructed to release the active drug by controlling the dissolution and / or diffusion of the active drug substance. Any of a number of methods can be implemented to achieve controlled release and a targeted plasma concentration versus time profile. In one example, controlled release is achieved by appropriate selection of various formulation parameters and ingredients, including, for example, various types of controlled release compositions and coatings. Thus, the drug is formulated into a pharmaceutical composition that releases the drug in a controlled manner when administered using an appropriate excipient. Examples include single or multiple unit tablet compositions or capsule compositions, oil solutions, suspensions, emulsions, microcapsules, microspheres, nanoparticles, patches and liposomes. Can be mentioned. In certain embodiments, the composition comprises a biodegradable pH sensitive and / or temperature sensitive polymer coating.

  Dissolution controlled or diffusion controlled release can be achieved by applying a suitable coating to the tablet, capsule, pellet or granule formulation of the compound or by incorporating the compound into a suitable matrix. it can. Controlled release coatings include one or more of the coating materials listed above, and / or, for example, shellac, beeswax, glycowax, hardened castor wax, carnauba wax, stearyl alcohol, mono Glyceryl stearate, glyceryl distearate, glycerol palmitostearate, ethyl cellulose, acrylic resin, dl-polylactic acid, cellulose acetate butyrate, polyvinyl chloride, polyvinyl acetate, vinyl pyrrolidone, polyethylene, polymethacrylic acid, methyl methacrylate, 2 -It may contain hydroxymethacrylate, methacrylate hydrogel, 1,3 butylene glycol, ethylene glycol methacrylate and / or polyethylene glycol. In controlled release matrix formulations, the matrix material can be, for example, hydrated methylcellulose, carnauba wax and stearyl alcohol, carbopol 934, silicone, glyceryl tristearate, methyl acrylate-methyl methacrylate, polyvinyl chloride, polyethylene and / or halogenated. Fluorocarbon and the like can be contained.

  Liquid forms for oral administration that can incorporate the compounds and compositions of the invention include aqueous solutions, appropriately flavored syrups, aqueous or oily suspensions, and edible oils (eg, cottonseed oil, sesame oil) , Coconut oil or peanut oil), and elixirs and similar pharmaceutical vehicles.

Coating Pharmaceutical compositions (e.g., tablets or capsules) formulated for oral delivery of the present invention are coated or formulated into dosage forms that provide delayed or extended release advantages. be able to. The coating can be adapted to release the active drug substance in a predetermined pattern (e.g., to achieve a controlled release formulation) or, e.g., an enteric coating (e.g., a pH sensitive polymer). (`` PH controlled release ''), polymers that have a slow rate of swelling, dissolution, or erosion or that have a pH-dependent rate of swelling, dissolution, or erosion (`` time-controlled release '') ), Polymers that are degraded by enzymes ("enzyme-controlled release" or "biodegradable release"), and polymers that form film layers that are destroyed by increasing pressure ("Pressure-controlled release") can be used to adapt to not release the active drug substance until it has passed through the stomach. The medical device described herein. Typical enteric coatings that can be used in a pharmaceutical composition include sugar coatings, film coatings (e.g., hydroxypropyl methylcellulose, methylcellulose, methylhydroxyethylcellulose, hydroxypropylcellulose, carboxymethylcellulose, acrylate copolymers, polyethylene glycols). And / or film coatings based on polyvinylpyrrolidone) or coatings based on methacrylic acid copolymers, cellulose phthalate acetate, hydroxypropylmethylcellulose phthalate, hydroxypropylmethylcellulose acetate succinate, polyvinyl acetate phthalate, shellac and / or ethylcellulose, etc. In addition, for example, glyceryl monostearate or distearies A time delay material such as glyceryl acid may also be used.

  For example, a tablet or capsule can include an inner dosage component and an outer dosage component, where the latter is in the form of a skin that encloses the former. The two components are enteric layers, where the enteric layers act against degradation within the stomach, allowing the internal components to enter the duodenum intact. Or can be delayed by release of the internal components).

  If an enteric coating is used, desirably a substantial amount of the drug is released in the lower gastrointestinal tract.

  In addition to coatings that provide delayed or prolonged release, solid tablet compositions are adapted to protect the composition from undesirable chemical changes (e.g., chemical degradation prior to releasing the active drug substance). Coatings may also be included. The coating can be applied to solid dosage forms in a manner similar to that described in “Encyclopedia of Pharmaceutical Technology, vols. 5 and 6, Eds. Swarbrick and Boyland, 2000”.

Formulations for releasing drug in the colon In some embodiments, a drug delivery system targeted to the colon can be used. Representative approaches include, but are not limited to:
(a) The drug is covalently bound to a carrier to form a prodrug that is stable in the stomach and small intestine and undergoes enzymatic conversion by the intestinal microflora in the large intestine to release the drug. Examples of such prodrugs include azo-conjugates, cyclodextrin-conjugates, glycoside-conjugates, glucuronate conjugates, dextran-conjugates, polypeptides and polymer conjugates. it can;
(b) approaches that deliver intact molecules to the colon, such as coating with a pH sensitive polymer that releases the drug at neutral or alkaline pH, or biodegradable that releases the drug upon degradation by bacteria in the colon Coating with polymer;
(c) embedding the drug in a biodegradable matrix and hydrogel that releases the drug in response to pH or biodegradation;
(d) time released systems (in this time release system, 3-5 hours after the multi-layer coated preparation has passed through the stomach (this corresponds to the time through the small intestine) The drug is released after a lag time has elapsed];
(e) the use of redox-sensitive polymers in which the combination of an azo polymer and a disulfide polymer releases the drug in response to the redox potential of the colon;
(f) the use of bioadhesive polymers that selectively adhere to the colonic mucosa and gradually release the drug; and
(g) Osmotic controlled drug delivery in which the drug is released through the semipermeable membrane due to osmotic pressure.

Parenteral administration Within the scope of the present invention are parenteral depot systems with biodegradable polymers. These systems release drugs that are injected or implanted into muscle or subcutaneous tissue and incorporated into the system over a long period of time ranging from days to months. Both the polymer characteristics and the device structure can control the release kinetics, which can be continuous or pulsatile. Polymer-based parenteral depot systems can be classified as implants or microparticles. The former is a cylindrical device that is injected into the subcutaneous tissue and the latter is defined as spherical particles in the range of 10-100 μm. Whereas implants are manufactured using extrusion, compression molding or injection molding, phase separation methods, spray drying methods and water-in-oil-in-water emulsion methods are often used for microparticles. The most commonly used biodegradable polymers for forming microparticles are polyesters derived from lactic acid and / or glycolic acid, i.e. poly (glycolic acid) and poly (L-lactic acid) (PLG / PLA micros). Sphere). Of particular interest are formed by in-situ depot systems such as thermoplastic pastes and gelling systems formed by solidification or cooling or by sol-gel conversion, cross-linking systems and amphiphilic lipids Organic gel. Examples of heat sensitive polymers used in the above systems include N-isopropylacrylamide, poloxamers (block copolymers of ethylene oxide and propylene oxide, such as poloxamer 188 and poloxamer 407), poly (N-vinylcaprolactam), poly Examples include (poly (siloethylene glycol)), polyphosphazene derivatives, and PLGA-PEG-PLGA.

Dosing regimen The method of the invention for treating chronic tissue ischemia is performed by administering a sufficient amount of inorganic nitrite for a period of time sufficient to effect neovascular growth in the ischemic tissue.

  The dosage and frequency of administration of the composition may vary depending on, for example, what is being administered, the condition of the patient and the method of administration. In therapeutic applications, the composition may be administered to a patient suffering from chronic tissue ischemia in an amount sufficient to reduce or at least partially reduce the symptoms of chronic tissue ischemia and its complications. . The dosage depends on the type and extent of progression of chronic tissue ischemia, the severity of chronic tissue ischemia, the age, weight and general health of the particular patient, the relative biological nature of the selected composition. It will depend on variables such as efficacy, excipient formulation, route of administration and judgment by the attending clinician. Effective doses can be extrapolated from dose-response curves derived from in vivo or animal model test systems. An effective dose is a dose that produces the desired clinical outcome, such as by ameliorating signs or symptoms of chronic tissue ischemia or slowing its progression.

  The amount of inorganic nitrite per dose can vary. For example, the subject can receive from about 0.1 μg / kg to about 10,000 μg / kg. Generally, the nitrite is administered in amounts that peak plasma concentrations range from 150 nM to 250 μM. Typical dosages can be between 0.1-5000 μg / kg, 100-1500 μg / kg, 100-350 μg / kg, 340-750 μg / kg or 750-1000 μg / kg. Typical dosages can be 0.25, 0.5, 0.75 or 1 mg / kg. Typical peak plasma concentrations can be 0.05-10 μM, 0.1-10 μM, 0.1-5.0 μM or 0.1-1 μM. The peak plasma concentration can be maintained for 6-14 hours (eg, 6-12 hours or 6-10 hours).

  The frequency of treatment can also vary. Subjects can be treated one or more times per day (e.g. once, twice, three times, four times or more times) or at specific times (e.g. about every 2 hours, every 4 hours, Every 6 hours, every 8 hours, every 12 hours or every 24 hours). Preferably, the pharmaceutical composition is administered 1-2 times per 24 hours. The time course of treatment can be of various durations, eg, 2 days, 3 days, 4 days, 5 days, 6 days, 7 days, 8 days, 9 days, 10 days or longer. For example, the treatment may be 2 times per day for 3 days, 2 times per day for 7 days, 2 times per day for 10 days. The treatment cycle can be repeated at intervals, eg, once a week, twice a month, or once a month, and the treatment cycle is separated by periods of no treatment. The treatment can be a single treatment or can continue for the lifetime of the subject (eg, for years).

Kits Any of the pharmaceutical compositions of the invention described herein can be used with a set of instructions, ie, can form a kit. The kit may contain instructions for using the pharmaceutical composition as a treatment described herein. For example, the instructions can provide dosing and treatment regimens for using the compounds of the invention to reduce chronic tissue ischemia.

Method of treatment
Nitrite plasma nitrite concentration as a supplement has been shown to have the highest number of risk factors and inversely correlates with cardiovascular risk factors in subjects with the lowest plasma nitrite concentrations (Kleinbongard et al ., Free Radical Biology & Medicine 40: 295-302,2006). In normal subjects, nitrite stored by exercise is released into the plasma, increasing the concentration of plasma nitrite; however, in diabetic and PAD patients, exercise increases the concentration of plasma nitrite. In practice, however, circulating nitrite concentrations are further reduced (Allen et al., Nitric Oxide 20: 231-237, 2009). Thus, nitrite supplementation can be achieved by the lack of plasma nitrite concentrations in cardiovascular and vascular disorders, and the lack of nitric oxide observed in the above diseases, given the relationship between nitrite and nitric oxide. It is considered effective in overcoming the lack of plasma nitrite concentration caused by dietary deficiency.

  The present invention relates to nitrites (eg, inorganic nitrites) or pharmaceutically acceptable prodrugs thereof for prophylactic and therapeutic nutrition, particularly in cardiovascular, metabolic, inflammatory or vascular diseases A nutritional composition of Specifically, the present invention relates to diabetes, peripheral arterial disease, chronic infection, acute infection, congestive heart failure, atherosclerotic cardiovascular disease, intermittent claudication, critical limb ischemic disease. ), Incomplete wound healing, stroke, myocardial infarction, inflammatory bowel disease, fracture, bone infection or peripheral neuropathy, stem cell disease and / or undernutrition observed in patients with dietary restrictions Relates to a novel composition of nitrite (eg, inorganic nitrite) or a pharmaceutically acceptable prodrug thereof that can be used to supplement Furthermore, the composition may also be used to treat undernourishment in patients suffering from a disease state that reduces plasma nitrite concentration or plasma nitric oxide concentration.

Inflammatory Diseases The pharmaceutical compositions and methods described herein can be used to treat congenital and acquired inflammatory diseases. Inflammatory diseases encompassed by the methods of the present invention can arise from a wide range of medical conditions that cause inflammation. One type of inflammatory disease that can be treated by the compositions and methods described in the present invention is an immune-inflammatory disease. Examples of immune-inflammatory diseases include rheumatoid arthritis, juvenile rheumatoid arthritis, osteoarthritis, transplant rejection, sepsis, acute respiratory distress syndrome, asthma and cancer. Another type of inflammatory disease that can be treated by the compositions and methods described in the present invention is an autoimmune disease. Examples of autoimmune diseases include conditions such as multiple sclerosis, psoriasis, inflammatory bowel disease, glomerulonephritis, lupus, uveitis and chronic hepatitis. Other inflammatory diseases can also be treated by the compositions and methods described in this invention, where such other inflammatory diseases include trauma, oxidative stress, cell death, radiation And conditions caused by injury, ischemia, reperfusion, cancer, transplant rejection and viral infection.

Tissue regeneration such as trauma, scarring, abnormal protein deposition, amyloidosis, ischemia or diabetes, infections or congenital abnormalities such as heart damage and gastrointestinal disorders that cause damage to the tissue or tissue damage After the tissue or organ is damaged due to the mold, the regeneration of the tissue can be stimulated using the pharmaceutical compositions and methods described herein.

Chronic tissue ischemia Chronic tissue ischemia is associated with a wide range of medical conditions that result in partial, substantially total or total reduction of blood flow to a body part or tissue containing a body part. Can be the result of disease, injury or unknown cause. Chronic tissue ischemia can also be affected by an individual's genetic makeup. Regardless of the medical condition leading to chronic tissue ischemia, patients suffering from chronic tissue ischemia may be treated with a pharmaceutically acceptable composition comprising an inorganic nitrite as described herein. It is a target. Treatment can completely or partially remove some or all signs and symptoms of chronic tissue ischemia, reduce the severity of the symptoms, and delay their onset Or the progression of symptoms that subsequently appear can be slowed or reduced in severity.

Neovascular Growth As described further below, the compositions of the invention are administered in a sufficient amount for a sufficient period of time to effect neovascular growth in ischemic tissue. The terms “new blood vessel growth”, “new blood vessel formation” and “new blood vessel development” can be used interchangeably. . Neovascular growth involves all phases of the process of angiogenesis, including initial signaling events, cellular recruitment of endothelial cells, formation and expansion of new blood vessels, and the connection of new and existing blood vessels. means. Neovascular growth can result from any process that results in vascular reconstruction or neovascularization of ischemic tissue (eg, angiogenesis, or arteriogenesis, or a combination of angiogenesis and arteriogenesis). The term “angiogenesis” is typically used to describe the embryonic development of blood vessels from hemangioblasts. Angiogenesis is generally understood to be a postnatal physiological process necessary for wound healing. Angiogenesis generally includes the formation of new capillaries or capillary branches by germination, budding and insertion growth from existing capillaries. Arteriogenesis, i.e., the growth of existing arteriole connections to the original collateral arteries, generally involves the formation of mature arteries from existing interconnecting arterioles after occlusion of the arteries. Understood. It shares some characteristics with angiogenesis, but the path to it and the end result may vary: arteriogenesis can potentially completely replace an occluded artery In contrast, angiogenesis generally cannot be so replaced. Even if the number of capillaries in the ischemic region is increased, blood flow cannot be increased if a limiting structure is present upstream of the new capillaries; Formation of new collateral vessels that bypass the bloodstream. In addition, the structures formed by angiogenesis and the structures formed by arteriogenesis differ in their cellular composition. Capillaries are tubes formed by endothelial cells supported by vascular pericytes. The arteries and veins are multi-layered (ie, the intima composed of endothelial cells, pericytes and basement membranes; the media, mainly composed of smooth muscle cells and their extracellular matrix; and the largest intravascular , A tube composed mainly of a fibroblast and its extracellular matrix, which is composed of an outer membrane).

Chronic tissue ischemia The method of the invention is characterized in that, as an underlying feature, blood flow to the tissue or organ is continuously reduced or blood flow to the tissue or organ is partially or completely blocked. It can be applied to any of a wide range of medical conditions. Thus, the method can be applied to the treatment of chronic tissue ischemia associated with disease, trauma or environmental stress. The decrease in blood flow to the tissue may be the result of progressive occlusion of the artery due to, for example, the presence of a clot or sclerosis and / or loss of elasticity due to atheromatous plaque. Reduced blood flow to the tissue can also be the result of environmental insults such as traumatic injury or surgery that blocks blood flow to the tissue or organ. Typically, the oxygen tension of the wound decreases rapidly and progressively, developing varying degrees of hypoxia throughout the wound area. Environmental conditions that cause hypoxia are also within the scope of the present invention.

  Examples of the disease included in the present invention include cardiovascular disease, peripheral arterial disease, arteriosclerosis, atherosclerotic cardiovascular disease, myocardial infarction, severe lower limb ischemic disease, stroke, acute coronary syndrome, intermittent There are lameness, diabetes including type 1 diabetes and type 2 diabetes, skin ulcer, peripheral neuropathy, inflammatory bowel disease, ulcerative colitis, Crohn's disease, intestinal ischemia and chronic mesenteric ischemia. The methods of the present invention can also be applied to chronic tissue ischemia associated with trauma (e.g., traumatic injury such as wounds, lacerations, burns, bruises, fractures or chronic infections). . Tissue damage received as part of a surgical procedure (eg, endarterectomy, etc.) is also encompassed by the present invention. Treatments involving tissue or organ transplants are also included within the scope of the present invention. Examples include vascular bypass transplantation, heart transplantation, liver transplantation, lung transplantation, islet cell transplantation, and transplantation of tissue generated in vitro for transplantation into a host. The methods of the present invention may include chronic ischemic conditions caused by exposure to environmental insults, such as prolonged exposure to hypoxic conditions (e.g., high altitude) or continuous aerobic exercise. It is also useful for treating chronic ischemic conditions caused by.

  The methods provided herein include a wide variety of types including, for example, muscle, smooth muscle, skeletal muscle, myocardium, nerve tissue, skin, mesenchymal tissue, connective tissue, gastrointestinal tissue or bone Can be applied to any organization. Soft tissue, epithelial tissue, such as single layer squamous epithelium, stratified squamous epithelium, cubic or columnar epithelium, loose connective tissue (also known as ring-shaped connective tissue), fibrous connective tissue, such as muscle bone Tendons to be connected to ligaments and ligaments that connect bones with joints.

  Thus, for example, peripheral arterial disease (PAD) (a form of peripheral vascular disease in which the artery is partially or completely blocked, usually vascular atherosclerosis leading to the leg or arm Symptoms of chronic tissue ischemia in (e.g.,) caused by intermittent claudication (i.e. fatigue, muscle spasm, hip movement, hip, hip, thigh, knee, shin or Upper foot pain), cladication during rest, numbness, tingling, lower legs or coldness in the legs, neuropathy, or tissue wound healing failure ( defective tissue wound healing). PAD in the lower limb is often associated with diabetes (particularly type 2 diabetes). Arm arterial disease is not usually due to atherosclerosis, but to other conditions such as autoimmune disease, blood clots, radiation therapy, Raynaud's disease, repetitive movements and trauma. Common symptoms when the arm is moving include discomfort, heavy feeling, fatigue, muscle cramps and finger pain. PAD can be diagnosed by performing one or more diagnostic tests including, for example, an ankle brachial blood pressure ratio (ABI) test, angiography, ultrasound or MRI analysis.

  Myocardial ischemia can have little or no symptoms, but is typically accompanied by symptoms such as angina, pain, fatigue and hypertension (fatigue elevated blood pressure). Diagnostic tests for myocardial ischemia include the following: angiography, resting electrocardiogram, exercise electrocardiogram or ambulatory electrocardiogram; scintigraphic study (radioactive heart scans) )); Echocardiography; coronary angiography; and, rarely, positron emission tomography.

  The method of the present invention also provides another therapy known in the art used to treat chronic tissue ischemia (where such therapy includes drug therapy, surgery, anti-inflammatory drugs, In combination with antibodies, exercise or lifestyle changes). The choice of a particular treatment can vary, and the choice will depend on the severity of chronic tissue ischemia, the subject's general health and the judgment of the attending clinician.

  The compositions of the present invention can also be formulated in combination with one or more additional active ingredients, where such additional active ingredients include any drug, such as antihypertensive. Examples include drugs, antidiabetic drugs, statins, antiplatelet drugs (clopidogrel and cilostazol), antibodies, immunosuppressive drugs, anti-inflammatory drugs, antibiotics, chemotherapeutic drugs, and the like. In some embodiments, the composition also contains inorganic nitrates; in other embodiments, the composition does not contain inorganic nitrates. For example, the composition of the present invention comprises inorganic nitrite and nitrates in a nitrite: nitrate ratio of 1-5 to 1-100, for example 1-5, 1-10, 1-30, 1-50, 1 It can be contained in a nitrite: nitrate ratio of -70 or 1-100.

Representative formulations for oral administration of controlled release pharmaceutical formulations include tablet formulations and capsule formulations. For example, it is possible to prepare capsule formulations using the powdered ingredients described for the tablet formulation, the appropriate dimensions of the capsule depending on the dose and packing density of the active ingredient, e.g. Size 1 capsule, size 0 capsule, size 00 capsule, etc. In some embodiments, tablets or capsules may not have an enteric coating. In another embodiment, the pharmaceutical composition of the present invention can be formulated to control release of nitrite ions. Where the capsule is described as being coated, the coating can be applied to the capsule after filling. Capsule formulations may optionally be self-locking capsule shells (e.g. `` Coni-Snap® '', `` Posilok® '') for ease of handling during the coating process. Alternatively, “Snap-Fit (registered trademark)” or the like can be used.

A typical composition contains 0.5 to 4.0 mmol of total nitrite ions (especially 1.8 to 3.6 mmol of NaNO ₂ ). The composition of any prodrug of such nitrite, for example, can contain NaNO _2, nitrite arginine KNO ₂ or 201~402mg of 154~308mg of 125～250Mg. The amount of nitrite ions used in the pharmaceutical composition can be varied as described herein. For example, the formulation can include an excipient as described herein, preferably an alkanizing agent (e.g., sodium bicarbonate or calcium carbonate), a glidant (e.g., fumed silica). Lubricants (fatty acid salts (e.g. magnesium stearate), pure solid fatty acids or solid polyethylene glycol) or bulking agents (e.g. silicified microcrystalline cellulose (Prosolv®) ) SMCC90)). The composition may also contain excipients described for use in compositions that are formulated for release in the intestine (eg, enteric preparations). The formulation also contains a rate-controlling polymer coating (eg, ethyl cellulose, cellulose acetate, cellulose acetate butyrate, cellulose triacetate, etc., which can be combined with PEG-4000). be able to. If desired, the amount of PEG-4000 used can be varied to produce aqueous pores in the coating through which sodium nitrite can diffuse. Enteric polymer coatings can also be used, and representative polymers include cellulose acetate phthalate (CAP), cellulose trimellitic acid, hydroxypropyl methylcellulose succinate acetate, `` Eudragit® L '' or `` Eudragit (registered trademark) S ". If a polymer coating is used, the formulation may also contain a plasticizer (such as triethyl citrate, triacetin or acetyl monoglycerides). A comprehensive enteric coating (polymer + plasticizer) can be added, for example in an amount of 10% by weight.

  The manufacture and testing of several tablet and pellet formulations for controlled release of nitrate are described below.

Tablet Preparation Method All solid ingredients including sodium nitrite were weighed to produce tablets with the desired weight ratio of ingredients. A sufficient amount of powder blend was prepared to prepare 4-5 tablets. The powdery ingredients were mixed thoroughly and then compressed into tablets. For tablets containing a waxy ingredient (i.e., Castorwax®), the mixture is dispersed while dispersing sodium nitrite and other ingredients in the molten wax and mixing to maintain a homogeneous blend. Solidified. After solidification, the mixture was pulverized into a powder for further mixing as needed. All powdery ingredients were mixed using a mortar and pestle.

  The tablets were compressed on a “Carver® Press” with 1/2 ”(1.27 cm) perforations and die. A force of 5000 lbs was applied for 30 seconds to obtain a tablet for release testing.

The tablet dimensions were as follows:
580mg tablet: 1.27cm (diameter) x 0.38cm (thickness) (1/2 "x 1/7"); or
480 mg tablet: 1.27 cm (diameter) x 0.32 cm (thickness) (1/2 "x 1/8").

  The tablet thickness was dependent on the total weight of the powdered ingredients and the nature of the excipients used. Thus, the disclosed thicknesses varied between 10-15% depending on the mixture being compressed.

  After compression, the tablets were carefully extruded from the die and stored in a desiccator until dissolution testing. Some tablets were coated with a controlled release or enteric coating material to change its release profile.

Preparation method of pellets For animal studies (oral administration to rabbits), small pellets containing 5 mg of sodium nitrite were prepared according to the following method. All solid ingredients, including sodium nitrite, were weighed to produce pellets in the desired weight ratio of the ingredients. A sufficient amount of powder blend was prepared to prepare 40-50 pellets. The powdery component was passed through a sieve (150-250 microns), mixed well by geometric dilution, and then compressed into a pellet. The pellet was compressed using a “Parr Model 2811 pellet press” with 3 mm perforations and a die. The compression of the pellets was done by manual compression and the applied force could not be controlled, but produced viscous pellets for all formulations. The weight of the pellet was 23-35 mg depending on the formulation used. One pellet batch was manually coated with an ethylcellulose / triacetin coating (4/1) that was 11-15% of the weight of the pellet.

  The dimensions of the pellets were as follows: 3 mm (diameter) x 5-7 mm (thickness). The thickness of the pellet depended on the total weight of the powdered ingredients and the nature of the excipients used. Thus, the disclosed thickness varied by about 50% depending on the mixture being compressed.

  After compression, the pellets were carefully extruded from a die and stored in a desiccator until shipped for animal testing. One pellet batch was coated with a controlled release coating to change its release profile. The coating method is described independently below. Castorwax pellets were compressed twice. The first compression was performed at ambient temperature and the second compression was performed in a 3 mm die after heating the die to 50-60 ° C. in an oven. The second compression induced good fluidity of Castorwax covering the sodium nitrite and sodium acetate particles.

Tablet / Pellet Coating Method Manually coat sodium nitrite tablets by carefully dropping a measured volume of the coating solution onto the surface of the tablet and carefully spreading the dripped coating solution over the surface and edges of the tablet. did. After evaporating the solvent, the above process was repeated many times until a sufficient amount of coating was applied. For pellets and some tablet batches, a dip coating method was used which involves carefully dipping the pellet / tablet into the coating solution and allowing it to air dry while being held with forceps. The dipping method was repeated until a sufficient amount of coating was applied.

  The coatings used were ethyl cellulose (EC) with triacetin as plasticizer and cellulose acetate phthalate (CAP, Cellacefate, NF). Different ratios of EC and triacetin were used to obtain coatings with different vulnerabilities and different permeability to water and sodium nitrite. EC / triacetin was coated onto tablets or pellets from solutions containing chloroform, methylene chloride or 95% ethanol. CAP was used as an enteric coating material and was coated onto tablets from dioxane solution. CAP coated tablets obtained with another coating solvent could not tolerate simulated gastric acid for 2 hours without disintegrating.

Tablet ingredients • Sodium nitrite, Certified ACS Reagent, Crystalline, Fisher Scientific, Lot # 080939A;
Polyox® Coagulant, Blend # C-289, molecular weight 5 million, NF Grade, Union Carbide;
Polyox (registered trademark) WSR 303, molecular weight 7 million, NF Grade, Colorcon;
Avicel® PH-302, microcrystalline cellulose, FMC Corporation, Lot # Q939C;
Ethocel®, ethyl cellulose, Standard 100 premium, Colorcon;
Castorwax®, NF, hydrogenated castor oil, CASCHEM, Lot # 00121431;
Methocel (registered trademark) K100M, hydroxypropyl methylcellulose, premium CR grade, Colorcon;
Klucel® HXAF Pharm., Hydroxypropylcellulose, molecular weight 1.15 million, Aqualon Division, Hercules, Inc .;
Klucel® MF Pharm., Hydroxypropylcellulose, molecular weight 850,000, Aqualon Division, Hercules, Inc .;
・ Sodium chloride, Certified ACS Reagent, Fisher Scientific;
• Sodium acetate trihydrate, ACS Reagent, Fisher Scientific.

Release Test Methods for Tablets All nitrite release tests used the USP paddle method with 50 RPM agitation. A Vankel® USP 6-station dissolution apparatus was used. A volume of 500 mL of distilled water at 37 ° C. was used as the release medium in each discharge vessel. The tablet release test was performed in duplicate or triplicate for each test formulation.

  A sample (35 mL) of the release medium was taken from each container at regular intervals (typically 1/2 hour, 1 hour, 2 hours, 3 hours, 4 hours, or longer). 35 mL of distilled water was added to the collected release medium.

  At the end of the release test, the tablet was crushed and the sodium nitrite contained in its dissolved state was completely released to determine the total sodium nitrite content in the tablet.

Sodium nitrite release assay
The UV absorbance at 355 nm was measured for each emitted sample in a 10-cm quartz cuvette using a Hewlett-Packard® 8453 diode array UV-visible spectrophotometer.

  Based on the calibration plots prepared in advance, the concentration of sodium nitrite in each sample was calculated and converted to the total amount and percent released for each tablet. The mean percentage released and the standard deviation were calculated for 2 or 3 tablets tested simultaneously. For each formulation, the average percent released was plotted against the time profile.

The formulations and release profiles of tablets and pellets produced by the above method are shown in Tables 1-7.

Formulation 9C is the same as Formulation 9, except that a 13% coating of ethylcellulose 100 / triacetin (1/10) was applied to the tablet from a 95% ethanol solution.

Formulation 200A was compressed twice. Initial compression was performed at ambient temperature. The second compression was performed in a 3 mm die after heating the die to 50-60 ° C. in an oven. Formulation 300A was dip coated using an ethylcellulose 100 / triacetin (4/1) coating solution with 95% ethanol as solvent.

Formulation 12C is the same as Formulation 12 except that a 14.8% coating of ethylcellulose 100 / triacetin (1/10) was applied to the tablet from a 95% ethanol solution. Formulation 13, Formulation 15, Formulation 15C1 and Formulation 15C2 were prepared by incorporating sodium nitrite and other ingredients into molten Castorwax. The solidified molten mass was mixed, and then pulverized using a mortar and breast into a powder, and then compressed into tablets. Formulation 15C1 and Formulation 15C2 are the same as Formulation 15 except that a 9.6% coating (15C1) or 4.15% coating (15C2) of ethylcellulose 100 / triacetin (4/1) was applied to the tablet from chloroform.

  Formulation 10C has a 15.8% coating of ethylcellulose 100 / triacetin (1/10) applied to tablets from a 95% ethanol solution. Formulation 2 was prepared by mixing sodium nitrite with powdered ethyl cellulose (Ethocel® 100) and compressing the resulting blend into tablets. Formulation 5 was prepared by mixing sodium nitrite, powdered ethylcellulose (Ethocel® 100) and HPMC K100M and compressing the resulting blend into tablets. Formulation 17C contains hydroxypropylcellulose (Klucel MF) and has an 8.65% coating of ethylcellulose 100 / triacetin (4/1) applied from a chloroform solution.

Simulated experiment of nitrite plasma concentration derived from controlled release formulation Several types of the above formulations were subjected to a simulated experiment regarding the measurement of nitrite plasma concentration. The simulation estimates a mid-range pharmacokinetic constant and an 80 mg dose. Estimated PK parameters for NaNO ₂ are: half-life = 45 minutes; clearance = 60.375 L / hour; oral bioavailability = 100% (provided that formulation 27 (bioavailability = 27%) is excluded); delay time from administration to reach pH at which release can occur = 0.5 hour. The mock experiment is administered twice per day for the first 2 days. A concentration of 69 ng / mL is equivalent to 1 μM and a concentration of 138 ng / mL is equivalent to 2 μM. The results are shown in FIGS.

  For Formulation 1, Formulation 2, Formulation 5, Formulation 9, Formulation 10C, Formulation 12 and Formulation 12C, formulas that fit those profiles did not have a zero y-intercept. That is, at t = 0, the percentage released was a positive number (a constant in the fitting polynomial). For the purposes of the simulation, this was treated as an immediate release component and the fraction was estimated to be released uniformly over the first 10 minutes after the lag time had elapsed. Thus, the release rate profile shows a “spike” of release over 10 minutes, and the “% release” profile has a significantly different slope between the first 10 minutes and the remaining 8 hours of release. .

Enteric Coated Capsule Formulation In some embodiments, the pharmaceutical composition can be formulated as an enteric coated capsule. Tables 8 and 9 provide formulations for enteric coated capsule formulations.

  In this method, capsules were prepared by mixing sodium nitrite, microcrystalline cellulose and blue food color using standard mixing methods for powders. The mixed ingredients were manually filled into size # 1 capsule shells using a small capsule filling machine. The completed capsules were tested for weight deviation and content uniformity in order to meet the compendia requirements described in the capsule specifications.

  The filled capsules were placed in a “Procoater holder” with the cap side of each capsule facing up. The coating tray was filled with the coating solution until it was within 1 mm from the top edge. After each dip coating step, additional coating solution was added to the tray as needed.

  The cap side of the capsule was immersed in the coating solution and slowly removed from the coating solution. Excess coating solution was carefully wiped from the bottom of the capsule so that the dried coating was symmetrical on the coating cap. The capsule was placed in a holder on the drying tray for 1 hour. The coating step was repeated four more times for a total of 5 coatings.

  After the coating dries, place the holder containing the capsule on the reversal stand with the cap side down (body side up) and push the capsule to the lowest position using the coating tray cover . The body side of the capsule was immersed in the coating solution and slowly removed from the coating solution. Excess coating solution was carefully wiped from the bottom of the capsule so that the dried coating was symmetrical on the coating body. The capsule and holder were then placed on a drying tray for 1 hour. The coating step was repeated four more times for a total of 5 coatings.

  Enteric coated capsules were tested for sodium nitrate release. Uncoated capsules were dissolved in greater than 75% in 0.1 N HCl (1 L) at 37 ° C. for 60 minutes using the USP paddle method at 50 rpm. In 750 mL of 0.1N HCl, enteric coated capsules released less than 1% sodium nitrite using the USP paddle method at 50 rpm for 120 minutes at 37 ° C. After adding 250 mL of 0.2 M tribasic sodium phosphate to 750 mL of 0.1 N HCl solution to raise the pH of the solution to 6.8, enteric coated capsules were subjected to USP paddle method at 50 rpm. In addition, 15-16 pancreatin was added at 37 ° C., and over 60% of sodium nitrite was released in 60 minutes.

Pharmacokinetic study in rabbits New Zealand rabbits weighing 3.0-3.2 kg were used to subject the sustained release sodium nitrite formulation to pharmacokinetic analysis. 1 mL of blood was collected at 14 time points over 6 hours.

  Initially, each rabbit received 31 mg / kg ketamine with 2 mg / kg xylazine diluted in sterile normal saline i.m. At this time, a second i.m. injection of 0.5 mg / kg acepromazine was also made. When the rabbit lost consciousness, one ear was shaved with a clipper. The area where the catheter was inserted was disinfected with alcohol and a 22 gauge iv catheter was inserted into the middle ear artery. A straight injection port was added to seal the end of the catheter. Blood was collected using a 22 gauge needle, and immediately after that, 1 unit / mL heparin solution (500 μL) was allowed to flow through the catheter. This treatment of flowing heparin was used after every blood collection.

  After the first blood collection, an 18 Fr gavage tube (length 36 cm) was inserted into the rabbit esophagus. At the end of the gavage tube, a nitrite capsule was inserted and quickly pushed into the stomach with 15 mL of air. Three types of formulations (formulation 100A, formulation 200A, and formulation 300A) were tested. The gavage tube was then removed and the remaining blood was collected over the next 6 hours.

  The collected blood was equally divided and placed in a 1.5 mL microcentrifuge tube. To one aliquot, 100 μL of plasma nitrite stock solution was added immediately, and the other aliquot was centrifuged at 5,000 rpm for 2 minutes to separate the plasma, which was then combined with 200 μL of plasma nitrite stock solution. All samples were stored in liquid nitrogen until subjected to processing.

The plasma nitrite stock solution included:
7.85 g KFeCN + 25 mL PBS = 1;
66 mg NEM + 3 mL PBS = 2;
1.5 mL nonidet P40 = 3;
1 (21 mL) + 2 (2.5 mL) + 3 = nitrite stock solution.

  Total NOx in plasma was calculated as described below. The time course for each of the three test formulations is shown in FIG. In addition, the amount of free nitrite was calculated by treating the sample with 580 mM sulfanilamide in 1N HCl for 15 minutes. This treatment captures free nitrite leaving nitrates, nitrosothiols, nitrosohemes and nitrosamines. The amounts of these residual components were measured by the method described below and these amounts are shown in FIG. If this amount is subtracted from the total NOx amount, the resulting numbers indicate the amount of free nitrite (FIG. 13). Data for Formulation 200A and Formulation 300A represent the average value of 5 rabbits and data for Formulation 100A represents the average value of 4 rabbits. This is because one rabbit receiving formulation 100A experienced clogging of the arterial catheter during the study.

Using nitric oxide chemiluminescent detection "Sievers 280i Nitric oxide analyzer (NOA)", to construct a standard curve for nitrite / NO concentration, and, the total NOx sample, nitrosothiols (SNO) + Nitorosohemu + nitrates Samples and free nitrite samples were measured. To measure nitrite, the purge vessel contained a reducing agent (2 mL sodium iodide in 7 mL glacial acetic acid) to reduce the nitrite, nitrate and nitroso compounds to free nitric oxide. The NO gas is then detected with NOA through a reaction with ozone, which emits photons of light detected with a chemiluminescence detector. The amount of NO present is determined by integrating the emission signal over time and the known amount of sodium nitrite (0 μM, 0.1 μM, 0.5 μM, 1 μM, 10 μM) as the source standard for NO. And 100 μM). Plasma nitrite was measured by reacting an aliquot of plasma with 580 nM sulfanilamide in 1N HCl for 15 minutes to capture free nitrite. The total amount of free nitrite was determined by subtracting the sulfanilamide value from the total NOx value.

Alternative Embodiments Although the invention has been described with reference to specific embodiments of the invention, further modifications are possible and all variations of the invention in which the application generally follows the principles of the invention. Use or adaptation (wherein such variations, uses or adaptations apply to the essential features described above, which are known or customarily practiced within the scope of the invention) It will be understood that it is intended to encompass (including what is not included in this disclosure).

  All references, patents, patent application publications and patent applications cited therein are incorporated herein by reference as if each of those references, patents, patent application publications and patent applications were incorporated by reference. As incorporated herein by reference to the same extent.

  “Claims” are as follows.

Claims (10)

Inorganic nitrite or a pharmaceutically acceptable salt of 40Mg～100mg, a sustained release pharmaceutical composition comprising 及 beauty pharmaceutically acceptable excipient, wherein the inorganic nitrite administration to humans the pharmaceutical compositions or a pharmaceutically acceptable salt is gradually released over 6-12 hours, the pharmaceutical compositions are formulated as solid dosage forms for oral administration, more given throw to the person of the pharmaceutical composition The composition wherein the plasma concentration of nitrite ions is maintained between 0.1 μM and 5.0 μM for 4-14 hours .   The pharmaceutical composition according to claim 1, wherein the period during which the plasma concentration is maintained occurs after a time when the plasma concentration is at its peak.   The pharmaceutical composition according to claim 1, wherein 30-50% of the nitrite ions are released in the first hour and the remainder of the nitrite ions are released in the subsequent 2-14 hours. The pharmaceutical composition according to claim 1, wherein the inorganic nitrite is administered at a dose of 0.05 mg to 10 mg per kg human body weight. Further comprising a pharmaceutically acceptable excipient for delaying release of the inorganic nitrite, whereby when orally administered to said human, substantially released inorganic nitrite in the stomach of the human The pharmaceutical composition according to claim 1 , which is not. A pharmaceutical composition according to claim 1 ,
And further include enteric or delayed release coating layer,
Here, the pharmaceutical composition, the when administered to human, so as not to be substantially released inorganic nitrite in the stomach of the human, is formulated, the pharmaceutical compositions. The pharmaceutical composition according to claim 1 for treating or preventing chronic tissue ischemia in humans. The pharmaceutical composition according to claim 1, for compensating for the shortage of circulating nitrite found in the human body. The nitrite ion is NaNO ₂ The pharmaceutical composition according to claim 1, provided as   The pharmaceutically acceptable excipient is methacrylic acid copolymer, polyox water-soluble resin, cellulose acetate phthalate, cellulose acetate trimellitic acid, polyvinyl acetate phthalate, hydroxyethyl cellulose phthalate, hydroxypropyl cellulose, ethyl cellulose / triacetin, sodium acetate 2. The pharmaceutical composition according to claim 1, selected from the group consisting of hydrogenated castor oil, and hydroxypropylmethylcellulose phthalate, shellac, or an aqueous dispersion thereof.

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